Extracellular Potassium Modulation of Drug Block of I Kr

Abstract

Background Torsade de pointes often occurs with underlying hypokalemia and bradycardia. A common effect of many drugs producing torsade de pointes is block of the rapidly activating component of the cardiac delayed rectifier (I_Kr). In this study, we evaluated the effect of changing extracellular potassium ([K⁺]_o) on I_Kr block by the nonspecific agent quinidine and by the specific I_Kr blocker dofetilide. Methods and Results I_Kr was measured in AT-1 cells, where contaminating outward currents are absent. The drug concentration producing 50% inhibition of I_Kr tails (IC₅₀) was strikingly [K⁺]_o-dependent. Elevating [K⁺]_o from 1 to 8 mmol/L increased the IC₅₀ for dofetilide block from 2.7±0.9 to 79±32 nmol/L and for quinidine block from 0.4±0.1 to 3.8±1.2 μmol/L. Conclusions (1) The increase in drug block with low [K⁺]_o provides a mechanism to explain the link between hypokalemia and torsade de pointes. (2) Elevations in [K⁺]_o occur with myocardial ischemia and with rapid pacing. Possible consequences of blunted drug block with high [K⁺]_o include loss of drug efficacy with ischemia and with rapid pacing; the latter may contribute to “reverse use-dependent” action potential prolongation. Extracellular potassium is a critical determinant of drug block of I_Kr, with substantial clinical implications.